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X 染色体上 1.1Mb 的片段缺失导致雄性小鼠减数分裂失败。

A 1.1-Mb segmental deletion on the X chromosome causes meiotic failure in male mice.

机构信息

Center for Animal Transgenesis and Germ Cell Research, Department of Animal Biology, University of Pennsylvania School of Veterinary Medicine, Philadelphia, Pennsylvania, USA.

出版信息

Biol Reprod. 2013 Jun 27;88(6):159. doi: 10.1095/biolreprod.112.106963. Print 2013 Jun.

Abstract

The mammalian X chromosome contains a large number of multicopy genes that are expressed during spermatogenesis. The roles of these genes during germ cell development and the functional significance of gene multiplication remain mostly unexplored, as the presence of multicopy gene families poses a challenge for genetic studies. Here we report the deletion of a 1.1-Mb segment of the mouse X chromosome that is syntenic with the human Xq22.1 region and contains 20 genes that are expressed predominantly in testis and brain, including three members of the nuclear export factor gene family (Nxf2, Nxf3, and Nxf7) and five copies of preferentially expressed antigen in melanoma-like 3 (Pramel3). We have shown that germline-specific Cre/loxP-mediated deletion of this 1.1-Mb segment is efficient and causes defective chromosomal synapsis, meiotic arrest, and sterility in male mice. Our results demonstrate that this 1.1-Mb region contains one or more novel X-linked factors that are essential for male meiosis.

摘要

哺乳动物 X 染色体包含大量在精子发生过程中表达的多拷贝基因。这些基因在生殖细胞发育中的作用以及基因倍增的功能意义在很大程度上仍未得到探索,因为多拷贝基因家族的存在给遗传研究带来了挑战。在这里,我们报告了小鼠 X 染色体上一个 1.1-Mb 片段的缺失,该片段与人类 Xq22.1 区域同源,包含 20 个主要在睾丸和大脑中表达的基因,包括核输出因子基因家族(Nxf2、Nxf3 和 Nxf7)的三个成员和黑色素瘤样 3(Pramel3)的五个拷贝。我们已经表明,这种 1.1-Mb 片段的生殖系特异性 Cre/loxP 介导缺失是有效的,并导致雄性小鼠的染色体联会、减数分裂阻滞和不育。我们的结果表明,这个 1.1-Mb 区域包含一个或多个对雄性减数分裂至关重要的新的 X 连锁因子。

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